Evidence that mutations in a loop region of the alpha-subunit inhibit the transition from an open to a closed conformation in the tryptophan synthase bienzyme complex

Evidence that mutations in a loop region of the alpha-subunit inhibit the transition from an open to a closed conformation in the tryptophan synthase bienzyme complex

Rapid-scanning stopped-flow (RSSF) UV-visible spectroscopy has been used to investigate the effects of single amino acid mutations in the alpha-subunit of the Salmonella typhimurium tryptophan synthase bienzyme complex on the reactivity at the beta-subunit active site located 25 to 30 A distant. The...

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Veröffentlicht in:The Journal of biological chemistry 1992-06, Vol.267 (18), p.13028-13038
Hauptverfasser: BRZOVIC, P. S, SAWA, Y, HYDE, C. C, MILES, E. W, DUNN, M. F
Format: Artikel
Sprache:eng
Schlagworte:
Allosteric Regulation
alpha subunit
Analytical, structural and metabolic biochemistry
Base Sequence
beta subunit
Binding Sites
biological activity
Biological and medical sciences
DNA
Enzymes and enzyme inhibitors
Fundamental and applied biological sciences. Psychology
Indoles - metabolism
Kinetics
Lyases
Models, Molecular
Molecular Sequence Data
Mutagenesis, Site-Directed
Protein Conformation
Salmonella typhimurium
Salmonella typhimurium - enzymology
site-directed mutagenesis
Spectrophotometry, Ultraviolet
tryptophan synthase
Tryptophan Synthase - chemistry
Tryptophan Synthase - genetics
Tryptophan Synthase - metabolism
U.V. spectroscopy
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Zusammenfassung:Rapid-scanning stopped-flow (RSSF) UV-visible spectroscopy has been used to investigate the effects of single amino acid mutations in the alpha-subunit of the Salmonella typhimurium tryptophan synthase bienzyme complex on the reactivity at the beta-subunit active site located 25 to 30 A distant. The pyridoxal 5'-phosphate (PLP) cofactor provides a convenient spectroscopic probe to directly monitor catalytic events at the beta-active site. Single substitutions of Phe for Glu at position 49, Leu for Gly at position 51, or Tyr for Asp at position 60 in the alpha-subunit strongly alter the observed steady state and pre-steady state inhibitory effects of the alpha-subunit-specific ligand alpha-glycerophosphate (GP) on the PLP-dependent beta-reaction. However, similar GP-induced allosteric effects on the distribution of covalent intermediates bound at the beta-site that are observed with the wild-type enzyme (Houben, K.F., and Dunn, M.F. (1990) Biochemistry 29, 2421-2429) also are observed for each of the mutant bienzyme complexes. These results support the hypothesis that the preferred pathway of indole from solution into the beta-site is via the alpha-site and the interconnecting tunnel (Dunn, M.F., Aguilar, V., Brzović, P., Drewe, W.F., Houben, K.F., Leja, C.A., and Roy, M. (1990) Biochemistry 29, 8598-8607). Residues alpha E49, alpha G51, and alpha D60 are part of a highly conserved inserted sequence in the alpha/beta-barrel topology of the alpha-subunit. We propose that the GP-induced inhibition of the beta-reaction results, in part, from a ligand-dependent conformational change from an "open" to a "closed" structure of the alpha-subunit which involves this region of the alpha-subunit and serves to obstruct the direct access of indole into the tunnel. Our findings suggest that the altered kinetic behavior observed for the alpha-mutants in the presence of GP reflects an impaired ability of the modified bienzyme complex to undergo the conformational transition from the open to the closed form.
ISSN:0021-9258
1083-351X
DOI:10.1016/S0021-9258(18)42377-0